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首页> 外文期刊>Nucleic Acids Research >Binding of an RNA aptamer and a partial peptide of a prion protein: crucial importance of water entropy in molecular recognition
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Binding of an RNA aptamer and a partial peptide of a prion protein: crucial importance of water entropy in molecular recognition

机译:RNA适体与a病毒蛋白的部分肽的结合:水熵在分子识别中的至关重要

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It is a central issue to elucidate the new type of molecular recognition accompanied by a global structural change of a molecule upon binding to its targets. Here we investigate the driving force for the binding of R12 (a ribonucleic acid aptamer) and P16 (a partial peptide of a prion protein) during which P16 exhibits the global structural change. We calculate changes in thermodynamic quantities upon the R12-P16 binding using a statistical-mechanical approach combined with molecular models for water which is currently best suited to studies on hydration of biomolecules. The binding is driven by a water-entropy gain originating primarily from an increase in the total volume available to the translational displacement of water molecules in the system. The energy decrease due to the gain of R12-P16 attractive (van der Waals and electrostatic) interactions is almost canceled out by the energy increase related to the loss of R12-water and P16-water attractive interactions. We can explain the general experimental result that stacking of flat moieties, hydrogen bonding and molecular-shape and electrostatic complementarities are frequently observed in the complexes. It is argued that the water-entropy gain is largely influenced by the geometric characteristics (overall shapes, sizes and detailed polyatomic structures) of the biomolecules
机译:阐明伴随分子与靶标结合的整体结构变化的新型分子识别是一个中心问题。在这里,我们调查的驱动力的结合R12(核糖核酸适体)和P16(a病毒蛋白的部分肽),其中P16表现出整体的结构变化。我们使用统计机械方法结合水分子模型来计算R12-P16结合后热力学量的变化,该模型目前最适合于生物分子的水合研究。结合是由水熵增益驱动的,该熵主要来自可用于系统中水分子平移位移的总体积的增加。与R12-水和P16-水吸引力相互作用的损失有关的能量增加几乎抵消了由于R12-P16吸引力(范德华和静电)相互作用获得的能量减少。我们可以解释一般的实验结果,即在配合物中经常观察到平面部分的堆积,氢键以及分子形状和静电互补性。有人认为,水的熵增益在很大程度上受生物分子的几何特征(整体形状,大小和详细的多原子结构)影响

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